OSU-03012, Hydrochloride Salt，≥99% 

【英文同義名】：AR-12 hydrochloride, OSU 03012, OSU03012

【中文同義名】：

訂購信息：（*，常備現(xiàn)貨）

產(chǎn)品描述

是OSU-03012的鹽酸鹽，OSU-03012是一種可口服的，PDK-1抑制劑，IC₅₀為5μM，并且比OSU-02067要高出2倍的效能^[1]。體外研究證明OSU-03012能抑制Huh7, Hep3B和HepG2等細胞系的生長。OSU-03012還能夠通過抑制PDK/AKT信號通路，誘導非小細胞肺癌和乳腺癌細胞的凋亡^[2,3,4]。另外，體內(nèi)研究顯示，OSU-03012具有良好的耐受性并在九周后抑制了55%的HMS-97神經(jīng)鞘瘤移植瘤的生長。因此，OSU-03012被認為是一種潛在VS和惡性神經(jīng)鞘瘤的化學治療藥物 ^[5]。

靶點

化學特性

結構式

Reference

[1]Zhu J, et al. From the Cyclooxygenase-2 Inhibitor Celecoxib to a Novel Class of 3-Phosphoinositide-Dependent Protein Kinase-1 Inhibitors.Cancer Res, 64(12), 4309-4318(2004).

[2] Gao M, et al. OSU-03012, a novel celecoxib derivative, induces reactive oxygen species-related autophagy in hepatocellular carcinoma. Cancer Res. 68(22):9348-57(2008).

[3] Wang YC, et al. Targeting endoplasmic reticulum stress and Akt with OSU-03012 and gefitinib or erlotinib to overcome resistance to epidermal growth factor receptor inhibitors. Cancer Res. 68(8):2820-30(2008).

[4] Kucab JE, et al. Celecoxib analogues disrupt Akt signaling, which is commonly activated in primary breast tumours. Breast Cancer Res. 7(5):R796-807(2005).

[5] Lee TX, et al. Growth inhibitory and anti-tumour activities of OSU-03012, a novel PDK-1 inhibitor, on vestibular schwannoma and malignant schwannoma cells. Eur J Cancer. 45(9):1709-20.